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- Title
Gene Expression Profiling in Pediatric Appendicitis.
- Authors
Dhillon, Bhavjinder K.; Kortbeek, Simone; Baghela, Arjun; Brindle, Mary; Martin, Dori-Ann; Jenne, Craig N.; Vogel, Hans J.; Lee, Amy H. Y.; Thompson, Graham C.; Hancock, Robert E. W.
- Abstract
Key Points: Question: What blood-based mechanistic changes distinguish pediatric patients with perforated appendicitis (PA) from those with simple appendicitis on presentation to the emergency department? Findings: This diagnostic study of 71 patients with pediatric appendicitis using systems immunology methods revealed a mechanistic understanding of severe disease, wherein a central role of immune dysregulation was observed with similarities to the mechanisms underlying sepsis. A blood-based gene expression signature of PA was also derived, providing a potential diagnostic for pediatric PA. Meaning: Development of early diagnostics and management strategies for pediatric PA should be informed by underlying immune dysregulation and similarities to sepsis. This diagnostic study evaluates mechanistic differences in disease severity in pediatric appendicitis. Importance: Appendicitis is the most common indication for urgent surgery in the pediatric population, presenting across a range of severity and with variable complications. Differentiating simple appendicitis (SA) and perforated appendicitis (PA) on presentation may help direct further diagnostic workup and appropriate therapy selection, including antibiotic choice and timing of surgery. Objective: To provide a mechanistic understanding of the differences in disease severity of appendicitis with the objective of developing improved diagnostics and treatments, specifically for the pediatric population. Design, Setting, and Participants: The Gene Expression Profiling of Pediatric Appendicitis (GEPPA) study was a single-center prospective exploratory diagnostic study with transcriptomic profiling of peripheral blood collected from a cohort of children aged 5 to 17 years with abdominal pain and suspected appendicitis between November 2016 and April 2017 at the Alberta Children's Hospital in Calgary, Alberta, Canada, with data analysis reported in August 2023. There was no patient follow-up in this study. Exposure: SA, PA, or nonappendicitis abdominal pain. Main Outcomes and Measures: Blood transcriptomics was used to develop a hypothesis of underlying mechanistic differences between SA and PA to build mechanistic hypotheses and blood-based diagnostics. Results: Seventy-one children (mean [SD] age, 11.8 [3.0] years; 48 [67.6%] male) presenting to the emergency department with abdominal pain and suspected appendicitis were investigated using whole-blood transcriptomics. A central role for immune system pathways was revealed in PA, including a dampening of major innate interferon responses. Gene expression changes in patients with PA were consistent with downregulation of immune response and inflammation pathways and shared similarities with gene expression signatures derived from patients with sepsis, including the most severe sepsis endotypes. Despite the challenges in identifying early biomarkers of severe appendicitis, a 4-gene signature that was predictive of PA compared to SA, with an accuracy of 85.7% (95% CI, 72.8-94.1) was identified. Conclusions: This study found that PA was complicated by a dysregulated immune response. This finding should inform improved diagnostics of severity, early management strategies, and prevention of further postsurgical complications.
- Subjects
CANADA; APPENDICITIS treatment; APPENDICITIS diagnosis; RESEARCH funding; ABDOMINAL pain; SEVERITY of illness index; DESCRIPTIVE statistics; TRANSCRIPTION factors; IMMUNE system; CLINICAL pathology; PEDIATRICS; LONGITUDINAL method; PERIPHERAL circulation; GENE expression profiling; CONFIDENCE intervals; INFLAMMATION; EVALUATION
- Publication
JAMA Pediatrics, 2024, Vol 178, Issue 4, p391
- ISSN
2168-6203
- Publication type
Article
- DOI
10.1001/jamapediatrics.2023.6721